TY - JOUR
T1 - Age- and tissue-specific changes in mitochondrial and nuclear DNA base excision repair activity in mice
T2 - Susceptibility of skeletal muscles to oxidative injury
AU - Szczesny, Bartosz
AU - Tann, Anne W.
AU - Mitra, Sankar
N1 - Funding Information:
This work is supported by UTMB Claude D. Pepper Older Americans Independence Center NIH Grant # P30 AG024832 (pilot grant to B.Sz.) and NIH P01 AG10514 and R01 CA53791 (to S.M.). We thank Sarah Toombs Smith for her suggestions to edit the manuscript.
PY - 2010/5
Y1 - 2010/5
N2 - In this study, we investigated age- and tissue-dependent changes in the DNA base excision repair (BER) of oxidative lesions in mitochondrial and nuclear extracts by measuring single-nucleotide (SN)- and long-patch (LP)-BER activities in five tissues isolated from 4-, 10- and 20-month-old mice. Age-dependent SN-BER and LP-BER activity was increased in the mitochondria of liver, kidney and heart, but generally decreased in skeletal muscles. In contrast, no significant changes in repair activity were observed in nuclear extracts of the same tissues, except for quadriceps, where the SN-BER activity was higher in the old animals. Moreover, the BER activities in both the nucleus and the mitochondria were significantly lower in skeletal muscles compared to liver or kidney of the same mice. The protein level of three antioxidant enzymes, Mn and Cu/Zn superoxide dismutases (SOD) and catalase, was also significantly lower in skeletal muscle compared to liver or kidney. In addition, we found higher levels of protein carbonylation in the mitochondria of skeletal muscle relative to other tissues. Thus, it appears likely that mouse skeletal muscle is highly susceptible to oxidative stress due to deficiency in both repair of oxidative DNA damage and antioxidant enzymes, contributing to age-dependent muscle loss.
AB - In this study, we investigated age- and tissue-dependent changes in the DNA base excision repair (BER) of oxidative lesions in mitochondrial and nuclear extracts by measuring single-nucleotide (SN)- and long-patch (LP)-BER activities in five tissues isolated from 4-, 10- and 20-month-old mice. Age-dependent SN-BER and LP-BER activity was increased in the mitochondria of liver, kidney and heart, but generally decreased in skeletal muscles. In contrast, no significant changes in repair activity were observed in nuclear extracts of the same tissues, except for quadriceps, where the SN-BER activity was higher in the old animals. Moreover, the BER activities in both the nucleus and the mitochondria were significantly lower in skeletal muscles compared to liver or kidney of the same mice. The protein level of three antioxidant enzymes, Mn and Cu/Zn superoxide dismutases (SOD) and catalase, was also significantly lower in skeletal muscle compared to liver or kidney. In addition, we found higher levels of protein carbonylation in the mitochondria of skeletal muscle relative to other tissues. Thus, it appears likely that mouse skeletal muscle is highly susceptible to oxidative stress due to deficiency in both repair of oxidative DNA damage and antioxidant enzymes, contributing to age-dependent muscle loss.
KW - Aging
KW - Base excision repair
KW - Mitochondria
KW - Oxidative stress
KW - Sarcopenia
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U2 - 10.1016/j.mad.2010.03.009
DO - 10.1016/j.mad.2010.03.009
M3 - Article
C2 - 20363243
AN - SCOPUS:77953036663
SN - 0047-6374
VL - 131
SP - 330
EP - 337
JO - Mechanisms of Ageing and Development
JF - Mechanisms of Ageing and Development
IS - 5
ER -